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首页> 外文期刊>Diabetes, metabolic syndrome and obesity: targets and therapy >MicroRNAs and Risk Factors for Diabetic Nephropathy in Egyptian Children and Adolescents with Type 1 Diabetes
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MicroRNAs and Risk Factors for Diabetic Nephropathy in Egyptian Children and Adolescents with Type 1 Diabetes

机译:埃及儿童和青少年糖尿病肾病的MicroRNA和患有1型糖尿病的危险因素

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Purpose: Currently available markers for early detection of diabetic nephropathy (DN), the leading cause of end stage renal disease, have some limitations. There is insufficient evidence from previous studies about the role of several circulating microRNAs (miRNAs) in the early development of DN. This study aimed to describe the expression of miRNA-377, miRNA-93, miRNA-25, miRNA-216a, and miRNA-21 in a sample of type 1 diabetic children and adolescents to explore their association with DN and some indices of kidney injury. Patients and Methods: Seventy type 1 diabetic patients, with 5 years’ duration of diabetes or more, were recruited from Children’s Hospital, Faculty of Medicine, Cairo University. Quantitative real-time reverse-transcription PCR (qRT-PCR) was used to measure the expression of the above mentioned miRNAs in serum and to assess its association with DN, and the studied risk factors. Results: There was a significantly higher percentage of up-regulation of miRNA-377 and miRNA-93 ( P =0.03, 0.02, respectively) in addition to significant down-regulation of miRNA-25 ( P =0.01) in patients with DN than in patients without DN. In patients with DN, expression of miR-216a was significantly negatively correlated with creatinine (r=? 0.4, P =0.04) and positively correlated with eGFR using creatinine (r=0.5, P =0.03). In the same group, expression of miR-21 was positively correlated with urinary cystatin C (r=0.6, P =0.01) and was negatively correlated with e-GFR using cystatin c (r=? 0.6, P =0.01). miRNA-93 was associated with increased risk (odds ratio=15, 95% CI=12.03– 24.63, P =0.01), while miRNA-25 was associated with decreased risk for albuminuria (odds ratio=0.15, 95% CI=0.08– 0.55, P =0.03). Conclusion: miRNA-377, miRNA-93, miRNA-216a, and miRNA-21 may be implicated in the pathogenesis of DN, while miRNA-25 may have a reno-protective role. More studies are needed to document the value of these miRNAs as diagnostic biomarkers as well as therapeutic targets in DN.
机译:目的:目前可用的标志物用于早期检测糖尿病肾病(DN),末期肾病的主要原因,有一些局限性。关于以前的几种循环微小RNA(miRNA)在DN早期发展中的作用的研究没有足够的证据。本研究旨在描述miRNA-377,miRNA-93,miRNA-25,miRNA-216a和miRNA-21在1型糖尿病儿童和青少年的样品中表达,以探索与DN和一些肾损伤指数的关联。患者和方法:七十型糖尿病患者,患有5年的糖尿病或更多糖尿病患者,来自开罗大学医学院的儿童医院招聘。定量实时逆转录PCR(QRT-PCR)用于测量血清中上述MIRNA的表达,并评估其与DN的关系,以及研究的危险因素。结果:除了DN患者中的MiRNA-25(P = 0.01)的显着下调除了患者之外,MiRNA-377和miRNA-93的上调百分比显着增加(p = 0.03,0.02),而不是在没有DN的患者中。在DN的患者中,miR-216a的表达与肌酐(r = 0.4,p = 0.04)显着呈负相关,并使用肌酐与EGFR呈正相关(r = 0.5,p = 0.03)。在同一组中,miR-21的表达与尿亚胱氨酰C(r = 0.6,p = 0.01)呈正相关,并且使用胱抑素C(r = 0.6,p = 0.01)与E-GFR负相关。 MiRNA-93与风险增加(差异= 15,95%CI = 12.03-24.63,P = 0.01)相关,而miRNA-25与白蛋白尿的风险降低有关(差价率= 0.15,95%CI = 0.08- 0.55,p = 0.03)。结论:miRNA-377,miRNA-93,miRNA-216a和miRNA-21可以涉及DN的发病机制,而miRNA-25可能具有肾上保护作用。需要更多的研究来记录这些miRNA的价值作为诊断生物标志物以及DN中的治疗靶标。

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